María J. Sancho scite author profile

Testosterone (40-300 microM), oestradiol (20-500 microM), progesterone (20-500 microM), dexamethasone (10 nM-1 microM) and corticosterone (1-10 microM) activate glycogen phosphorylase rapidly when added directly to hepatocytes. The activation of phosphorylase was concentration-dependent and occurred after 10 min for dexamethasone, 30 min for testosterone and 60 min for oestradiol and progesterone. This rapid effect does not appear to be dependent on a stimulation of protein synthesis, it is independent of an increase in cyclic AMP, and it is not diminished by the presence of ornithine decarboxylase inhibitors. The stimulation of phosphorylase activity is diminished by depleting the incubation medium of Ca2+ in the presence of 0.5 mM-EGTA, and therefore it may involve changes in the distribution of Ca2+ in the hepatocytes. These results may explain some of the pharmacological effects of sex steroids, and also might contribute to the physiological actions of glucocorticoids.

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Conventional and right‐sided screening for subcutaneous ICD in a population with congenital heart disease at high risk of sudden cardiac death

Alonso

Osca

Rueda

et al. 2017

Noninvasive Electrocardiol

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Effects and interaction studies of trifusal and other salicylic derivatives on cyclooxygenase in rats

Castellarnau¹,

Sancho²,

Vilá³

et al. 1988

Prostaglandins, Leukotrienes and Essential Fatty Acids

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An early effect of estradiol at hepatic level, previous to its protein synthesis activation

Sanchez-Bueno

Sancho

Trueba

et al. 1987

International Journal of Biochemistry

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María J. Sancho

Neurosteroids: Biosynthesis, metabolism and function of pregnenolone and dehydroepiandrosterone in the brain

Rapid activation of glycogen phosphorylase by steroid hormones in cultured rat hepatocytes

Conventional and right‐sided screening for subcutaneous ICD in a population with congenital heart disease at high risk of sudden cardiac death

Effects and interaction studies of trifusal and other salicylic derivatives on cyclooxygenase in rats

An early effect of estradiol at hepatic level, previous to its protein synthesis activation

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